Posttraumatic Stress Disorder (PTSD) Clinical Trial
Official title:
Brain Circuitry and Psychosocial Predictors of PTSD
To employ a fear learning-extinction paradigm with functional magnetic resonance imaging (fMRI) and skin conductance response (SCR) assessments among patients with posttraumatic stress disorder (PTSD) and trauma exposed healthy controls, aiming to a) clarify neural circuits underlying PTSD and b) to probe brain based predictors of symptomatic improvement in response to Prolonged Exposure (PE) treatment, and first line treatment for PTSD.
Posttraumatic stress disorder (PTSD) is highly prevalent and debilitating disorder. It is
defined by a fearful response to traumatic events, and its clinical picture includes
reexperiencing, arousal, and avoidance to reminders of the exposure. Despite efforts to
characterize the pathophysiology of PTSD, no biomarkers have been established that aid in
diagnosis, treatment development, or prediction of treatment response.
Several lines of evidence suggest that PTSD symptoms are mediated by dysfunctional processes
involving the brain's fear-circuitry network in general, and extinction learning and recall
deficits in particular. Based on our preliminary work in applying fear extinction task to
healthy humans and patients with PTSD the goal of this renewal RO1 application is to employ
an established extinction paradigm with functional magnetic resonance imaging (fMRI) and
Skin Conductance Response (SCR) assessments in a large and well characterized sample with
PTSD and trauma exposed healthy control (TE-HC) subjects. We plan to clarify circuits
underlying PTSD psychopathology and to probe, for the first time, neural circuitry of
symptomatic improvement in response to Prolonged Exposure (PE) treatment. This goal is
congruent with NIMH strategic plan strategy 1.3 ("identify and integrate biological markers
and behavioral indicators associated with mental disorders").
One hundred subjects including 60 individuals with a principal diagnosis of PTSD and 40
trauma exposed healthy controls will be assessed by fMRI and SCR to determine the neural
circuitry activation to the fear extinction task. fMRI data will be acquired simultaneously
with fear extinction and recall measurement quantified by SCR. All 60 PTSD subjects and 20
randomly assigned TE-HCs subjects will repeat these procedures 10 weeks later, after PTSD
subjects have completed 10 weeks of intensive PE treatment. Three months after treatment
completion clinical ratings of PTSD severity will be conducted to permit analysis of neural
predictors of long term treatment durability.
The aims above will be accomplished through four years of study, conducted by a
multi-disciplinary research team, comprised of research scientists from Columbia, Harvard
and New York Universities, who have conducted studies in PTSD and structural and functional
brain imaging. If successful, the study will produce highly needed information on the neural
circuitry which underlies deficient extinction and recall in PTSD, and will provide highly
important information about the neural effects of Prolonged Exposure treatment, a first line
treatment for PTSD. Together these lines of expected findings will not only advance
identification of biomarkers associated with PTSD, but also facilitate identification of
biomarkers for clinical reponse to an empirically supported treatment.
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Allocation: Non-Randomized, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Basic Science
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